首页> 外文期刊>The Journal of Nuclear Medicine >Detection of Secondary Thalamic Degeneration After Cortical Infarction Using cis-4-18F-Fluoro- D-Proline.
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Detection of Secondary Thalamic Degeneration After Cortical Infarction Using cis-4-18F-Fluoro- D-Proline.

机译:使用cis-4-18F-Fluoro-D-Proline检测皮质梗死后继发的丘脑变性。

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摘要

The amino acid cis-4-(18)F-fluoro-d-proline (d-cis-(18)F-FPro) exhibits preferential uptake in the brain compared with its l-isomer, but the clinical potential of the tracer is as yet unkown. In this study we explored the cerebral uptake of d-cis-(18)F-FPro in rats with focal cortical infarctions. METHODS: Focal cortical infarctions were induced in different areas of the cortex of 20 Fisher CDF rats by photothrombosis (PT). At variable time points after PT (1 d to 4 wk), the rats were injected intravenously with d-cis-(18)F-FPro. For comparison, 12 rats were injected simultaneously with (3)H-deoxyglucose ((3)H-DG), 3 rats were injected with (3)H-methyl-l-methionine ((3)H-MET), and 2 rats were injected with (3)H-PK11195. Within 2 h after injection of the tracers, coronal cryosections of the brains were produced and evaluated by dual-tracer autoradiography. Lesion-to-brain ratios (L/B ratios) were calculated by dividing the maximal uptake in areas with increased tracer uptake by the mean uptake in normalbrain tissue. Histologic slices were stained by toluidine blue and by immunostainings for glial fibrillary acidic protein (GFAP), CD68 for macrophages, and CD11b for microglia. RESULTS: Prominent uptake of d-cis-(18)F-FPro was found in ipsilateral thalamic nuclei (TN) and partially in the corpus striatum starting at 3 d after infarction with increasing L/B ratios up to 4 wk (mean L/B ratio +/- SD, 6.7 +/- 3.5). The involved TN varied with the site of the cortical lesion corresponding to their thalamocortical projections connecting them with their specific target region in the cerebral cortex. The TN were positive for CD11b and GFAP from day 7 onward, whereas uptake of (3)H-DG, (3)H-MET, and (3)H-PK11195 and immunostaining for CD68 were similar to that of normal brain. Furthermore, increased uptake of d-cis-(18)F-FPro was found in the area of the cortical infarctions (mean L/B ratio +/- SD, 12.1 +/- 8.1). From day 5 onward, the pattern of uptake was congruent with that of immunostaining for CD11b and CD68 but was different from that of GFAP. CONCLUSION: d-cis-(18)F-FPro appears to be a sensitive PET tracer for detection of secondary degeneration of TN after cortical injury. The uptake mechanisms of d-cis-(18)F-FPro remain to be elucidated, but the relationship to microglial activation suggests a diagnostic potential in various brain diseases.
机译:氨基酸cis-4-(18)F-氟-d-脯氨酸(d-cis-(18)F-FPro)与l-异构体相比,在大脑中具有优先摄取,但示踪剂的临床潜力是还不知道。在这项研究中,我们探索了局灶性皮层梗死大鼠的d-顺式-(18)F-FPro的脑摄取。方法:20只Fisher CDF大鼠的皮层不同区域通过光血栓形成(PT)诱发局灶性皮层梗死。在PT后(1 d至4 wk)的可变时间点,给大鼠静脉注射d-顺式-(18)F-FPro。为了比较,同时给12只大鼠注射(3)H-脱氧葡萄糖((3)H-DG),向3只大鼠注射(3)H-甲基-1-甲硫氨酸((3)H-MET),和2只给大鼠注射(3)H-PK11195。注射示踪剂后2小时内,产生了大脑的冠状冰冻切片,并通过双示踪放射自显影对其进行了评估。通过将示踪剂摄取增加的区域的最大摄取量除以正常大脑组织的平均摄取量来计算病变与大脑的比率(L / B比率)。组织切片用甲苯胺蓝染色,神经胶质原纤维酸性蛋白(GFAP)染色,巨噬细胞CD68,小胶质细胞CD11b染色。结果:梗死后3 d开始在同侧丘脑核(TN)和纹状体的一部分中摄取d-cis-(18)F-FPro,L / B比增加至4 wk(平均L / B比率+/- SD,6.7 +/- 3.5)。所累及的TN随皮质病变部位的变化而变化,而皮质病变部位的丘脑皮质投影将它们与大脑皮质中的特定目标区域连接起来。从第7天开始,TN对CD11b和GFAP呈阳性,而(3)H-DG,(3)H-MET和(3)H-PK11195的摄取以及对CD68的免疫染色与正常脑相似。此外,在皮质梗死区域发现d-顺式-(18)F-FPro的摄取增加(平均L / B比+/- SD,12.1 +/- 8.1)。从第5天开始,摄取模式与CD11b和CD68的免疫染色模式一致,但不同于GFAP。结论:d-顺式-(18)F-FPro似乎是一种灵敏的PET示踪剂,可检测皮质损伤后TN的继发性变性。 d-顺式-(18)F-FPro的摄取机制尚待阐明,但与小胶质细胞活化的关系表明在各种脑部疾病中都有诊断潜力。

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